DE2935901C2 - 1- (2-Acetylphenylthio) -3-alkylamino-2-propanols and their acid addition salts, processes for their preparation and medicaments containing them - Google Patents

Abstract

1. Claims for the contracting states BE, CH, LI, FR, GB, IT, LU, NL, SE 1-phenylthio-3-alkylamino-2-propanoles represented by the general formula I see diagramm : EP0025528,P9,F1 in which R1 is a straight chain or a branched C1 to C5 -alkyl or cycloalkyl group, and the physiologically acceptable acid addition salts thereof. 1. Claim for the contracting state AT A process for the production of 1-phenylthio-3-alkyl-amino-2-propanoles represented by the general formula I see diagramm : EP0025528,P10,F2 in which R1 is a straight chain or a branched C1 to C5 alkyl or cycloalkyl group, and its physiologically acceptable acid addition salts characterized in that, in a per se known manner, (a) an amine of the formula H2 N-R1 is reacted with an arylglycidsulfide represented by the general formula II see diagramm : EP0025528,P10,F3 or with a halogen hydrine represented by the general formula III see diagramm : EP0025528,P10,F4 wherein Hal is chlorine, bromine or iodine, or b) a thiophenole represented by the general formula IV see diagramm : EP0025528,P10,F5 is reacted with a compound of the formula X-CH2 -NH-R1 , wherein X represents the see diagramm : EP0025528,P11,F1 or Y-CH2 -CH(OH) group, wherein Y is a replaceable radical, or (c) a disulfide represented by the general formula V see diagramm : EP0025528,P11,F2 is under reducing conditions reacted with the partners indicated under (b), or (d) an amino derivative of the formula VI see diagramm : EP0025528,P11,F3 is allowed to react with an alkylhalogenide of the formula Hal-R1 , wherein R1 has the same meaning as in the general formula I.

Description

S-CH ₃ -CH-CHi-NH-R ₁
OH 0)

C-CH ₃

in the R | a straight or branched chain Cp bis Cä-alkyl or cycloalkyl group and their Physiologically acceptable acid addition salts that have 0-sympatholytic properties, which is why they are suitable for the treatment and prophylaxis of heart diseases and for combating hypertension.

The invention also relates to processes for the preparation of the compounds of the formula I and medicaments containing these, according to the preceding claims 2 and 3.

The compounds of the formula I can be prepared in various ways. A particularly suitable one The method consists in the implementation of an aryl glycide sulfide bull of general formula II

with a 1-halogeno-2-hydroxy-3-a | kylaminopropane of the general formula

X-CH2-CHOH-CH2-NH-R1,

in which X represents a halogen atom.

The reaction is carried out in the equivalent of a solvent and an acid-binding agent at temperatures of 70 - 120 ° C carried out under inert gas.

A variant of this method is the implementation of a disulfide of the general formula V,

S-S

(V)

S-CH ₂ -CH-
\

-CH ₂

C-CH ₃

Il ο

with an alkylamine of the general formula H ₂ N-Ri, where the radical Ri <J has the same meaning as in formula I. Preferred solvents are: alcohols, in particular ethanol or isopropanol, and cyclic ethers such as tetrahydrofuran or di> van, where the Reaction at temperatures of 70-120 ⁰ C and normal pressure is carried out.

Another type of preparation consists in the reaction of a halohydrine of the general formula III

S-CH ₂ -CH-CH ₂ -HaI

^Oh

C-CH ₃

(IV)

-CH,

under reducing conditions with the specified reactants. As a reducing agent are here preferably sodium borohydride, sodium dithionite or alkali metal sulfides in alcoholic or aqueous solution used

The compounds I can also be prepared

by reacting an amino derivative of the formula VI

S-CH ₂ -CH-CH ₂ -NH ₂

OH

(VD

C -CHj

Il ο

with an amine the more general! Formula H ₂ N-Ri. The reaction is expediently carried out in the presence or absence of a solvent at elevated temperatures under atmospheric pressure or under pressure in a closed vessel, if appropriate in the presence of an acid-binding agent. Preferred solvents are ethanol or isopropanol.

According to a further production method, the new substances can also be produced by condensation of a thiophenol of the general formula IV

with a compound of the formula Z-Ri (where Z = chlorine, bromine, iodine or the toluene-p-sulfonyloxy radical means). The reaction is preferably carried out in the presence of a base, e.g. B. sodium or Potassium carbonate in a solvent such as. B. ethanol or isopropanol, at an elevated temperature executed. The compounds according to the invention obtained are purified in the customary manner, for example by recrystallization from a

Solvent, conversion to an acid addition compound or by column chromatography.

The compounds of general formula I according to the invention contain an asymmetric carbon atom in the 2-position of the aliphatic side chain and are obtained as racemates by known Methods, for example via the formation of diastereomeric salts with optically active auxiliary acids, such as tartaric acid or camphor-IO-sulfonic acid, and its fractionators ter crystallization separated into the optical antipodes

$ 5 can be.

The compounds of the formula I can be mixed with physiologically acceptable acids in the customary manner Acid addition salts are produced. Suitable acids are e.g. B. Salt *, sulfur, phosphorus, vinegar, Lactic, maleic or fumaric acid.

The compounds of the formula I and their physiologically tolerable acid addition salts not previously described have valuable pharmacological properties. They can be used for the treatment and prophylaxis of heart and circulatory diseases.

From DE-AS 12 36 523 it was known that certain phenoxypropyl ethers anipyretic, analgesic

see and possess localistic properties. It is also already described there that basic 1-phenyl or 1-naphthyl ether and thioether des 2-Hydroxy-3-tert-butylaminopropane coronary dilator Have properties combined with a good sedative effect. Also in the DE-OS 14 93 848 is disclosed that such 1-Phenyläther or thioether of 2-hydroxy-3-aminopropane with a substituted amino group, which may optionally be on Phenyl radical through lower alkyl radicals or Halogenato- ι ο me can be substituted for the treatment or prophylaxis of coronary artery diseases are useful. In publication 11 Formaco Ed. Sc, Vol. 24, 1969, pp. 349-357 is reported by L Villa et al reports that phenoxy-hydroxyisorpopylaminopropane possesses 0-adrenolytic properties but it is Surprisingly that by a substitution on the phenylthioether group in 2-position with an acetyl test sine particularly strong and competitive / ϊ-receptor blocking Effect is achieved. Because of the particularly clear 0-sympatholytic self-activity These new compounds are particularly suitable for the treatment of coronary heart diseases and cardiac arrhythmias and hypertension.

The effectiveness of the compounds according to the invention as / J-blockers was determined by the following tests in Comparison to the most well-known compound of this group of substances introduced in practice »Propranolol« as well as for Practolol:

Attempt 1

The direct effect on the stroke frequency and contraction force as well as the effect on the increase in both parameters triggered by isoprenaline was investigated in vitro on the right, spontaneously beating, and left, electrically stimulated guinea pig atria (Pirbright White). The preparation of the atria was carried out according to HOLZ and WESTERMANN (Exp. Pathol. Pharmacol. 225, 421 (1955), the test arrangement according to WAGNER et al (Arzneimittel. Forsch. 22, 1061 (1972)). Those concentrations of the inventive Compound determined which reduced the isoprenaline effect (5.8 · ΙΟ- ⁹ molar in the right and 3.2 · 10 ~ ⁸ molar in the left atria) by half. The results obtained are shown in the table.

Attempt 2

To demonstrate the competitive 0-adrenergic antagonism in vivo, mixed-breed cats of both sexes ¹ »and η chloralose pentobarbital anesthesia were used. According to the method of ÄBLAD et al (Eur. J. Pharmacol. Π, 59 (1970)), a polyethylene catheter was inserted into the right femoral artery to measure the blood pressure. The registration took place via a Statham element from a Beckman Dynograph type R. The heart rate was taken from the blood pressure amplitude with the aid of a cardiotachometer and recorded on a further channel of the dynograph. The test solutions are applied via a catheter into the left femoral vein. The inhibiting effect of increasing test substance doses on the i, v. Administration of 0.5 μg isoprenaline / kg body weight tested for induced tachycardia or hypotension (lowering of blood pressure).

The doses of the reference compound or compound according to the invention were entered in the table as EDm values, which each reduced the isoprenaline effects by half.

Attempt 3

The sympathomimetic self-activity (ISA) was determined according to the method of BARRET & CARTER (Br. J. Pharmacol. 40, 373 (1970)) on pentobarbital anesthetized male Wistar rats. The animals received 5 mg / kg reserpine 24 hours before the start of the experiment intraperitoneally. The heart rate was determined from the blood pressure amplitude (polyethylene catheter with attached Statham element in the right femoral artery) removed with the aid of a cardiovascular meter and continuously registered on a recorder. The test solutions were applied using a Catheter in the left femoral vein. Four increasing doses of each test compound were separated each tested on six different animals

The maximum increase in heart rate (mean value from 6 animals) by the individual test compounds was taken as a measure of their agonistic activity and as a percentage of the increase in frequency by 1.0 μg isoprenaline / kg body weight i.a. v. calculated

The results obtained can be found in the table.

Attempt 4

The acute toxicity was determined in NMEI mice by intravenous or oral administration of increasing doses of the Determined compound according to the invention. The death rates were within the 7 day observation determined and the mean lethal dose determined

The results shown by way of example in the table show that the compounds according to the invention a strong competitive ß-receptor-blocking effect both on the isolated organ and on the genetic animal and thus a therapeutically useful protection against a pathologically increased sympatheticotinus deliver. A comparison with two known reference substances of this indication class can make this possible Clarify the statement, pointing out that propranolol is the most important and most common represents used medicinal products of this indication group.

The invention also has two connections known from DE-AS 12 36 523 The active ingredient has a significantly stronger effect, as the results of these comparisons show.

/ ο

Results of pharmacological and toxicological studies on the compound of the invention in the Comparison to two reference substances

attempt Isolated guinea pig application Propranolol Practolnl Ingenuity 54% 33 "« Forecourt Link') 1. Inhibition of isoprenaline IT) F-D ,,, *) ED ,,, *) LD ,,, *) LDV) induced increase in frequency 148 mg / kg 111 mg / kg 1.1. Inhibition of isoprenaline Organ bath 1.5 · 10 ⁷ molar 7.1 · 10 molar 2.6 · 10 'molar 2874 mg / kg 667 mg / kg induced contraction crart 1028 2523 12th increase Organ bath 4.5 · IO "molar 2.3 x 10 "molar 4.7 x 10 "molar Anesthetized cat Inhibition of isoprenaliri- 2. induced heart rate IT) IT) 1 D ", *) 2.1. increase intravenous 0.017 mg / kg 0.144 mg / kg 0.044 mg / kg Reserpinized rat (under anesthesia) ^ -sympathomimetic Eigen 3 activity (ISA) in% of the sympathomimetic activity of isoprenaline 3.1. acute toxicity intravenous O ¹ Vo mouse 4th mouse LD ,,, *) 4.1. "Therapeutic breadth" intravenous 40 mg / kg 4.2. Quotient of 4.1. : 2.1. orally 280 mg / kg S. 2353

Compound according to the invention: 1- (2-Acetylphenylthio) -tert-bulylamino-2-propanol HCI. Determined with the help of the probitanalysis.

Comparison of the compound according to the invention 1- (2'-acetylphenylthio) -3-tert-butylamino-2-propanol (Example 1) with two basic phenylthioether compounds of DE-AS 12 36 523 (comparison compound A- l-phenylthio-3-tert-butylamino-2-propanoI and comparison compound B: 1- (2-methylphenylthio-3-tert.-bj'ylamino-2-propanol)

Example !

Comparative compound A

Comparison compound B

Isolated guinea pig atrium

Inhibition of the isoprenaliri-induced increase in frequency

Inhibition of the isoprenaliri-induced increase in contraction force

ED; ,, ED ,,, ED ;,

2.6 · 10 "molar 3.6 · 10" molar 5.8 · 10 "molar

4.7 x 10 "" molar 4.4 x 10 "molar 6.4 x 10" molar

The compounds according to the invention can be administered in the customary application forms.

The therapeutic formulations are the usual Trägerstof ^f sn or diluents and pharmaceutical auxiliaries usually used depending on the type of administration with a suitable dosage in a known per se manner The preferred preparations consist in a form suitable for oral administration. Such dosage forms are z. B. tablets, film-coated tablets, coated tablets, capsules, pills or depot forms. Parenteral preparations, such as injection solutions, are also suitable.

The compounds according to the invention are described in more detail by the following examples.

The thiophenols used as starting materials are, if not specifically mentioned, by reduction the corresponding sulfonic acid chlorides or, according to Leuckart, via diazonium salt and xanthate from the Anilines produced.

Example I.

To a stirring solution of 15.1 g (0.1 mol) o-Mercaptoacetophenone in 100ml water and ig sodium hydroxide is at room temperature and below Nitrogen, 11.2 g (0.12 mol) of epichlorohydrin were added dropwise. An oil separates out immediately. After stirring for two hours, the mixture of epoxide and chlorohydrin becomes separated by extraction with 100 ml of chloroform, dried with anhydrous sodium sulfate and concentrated. 19.6 g of a bluish oil are obtained, which is reacted further without purification.

9.6 g of the mixture obtained, 20 ml of tert-butylamine and 50 ml of isopropanolol are refluxed for 15 hours. After evaporation in vacuo 25 g of a brown oil are obtained. It is dissolved in 120 ml of chloroform and three times with 50 ml of 4N HCl extracted. The aqueous phase is made alkaline and extracted twice with 100 ml of ethyl acetate each time. The combined extracts are washed.

ίο

dried and concentrated under reduced pressure. 15 g of 1- (2'-acetylphenylthio) -3-tert-butylamino-2-propanol are obtained obtained as a brownish oil. The base, dissolved in isopropanol, is added dropwise brought to crystallization by ethereal HCI. The salt is suctioned off and recrystallized again Isopropanol provides the pure hydrochloride.

Yield: 11.5 g, mp: 156-8 °.

The following compounds are made according to the methodology of Example I:

Examples

Fp (IICI)

Isopropyl 182-183 ° Cyclopentyl 180-182 ° sec-butyl 125-127 ° Cydopropyl 183-186 °

Claims (3)

Patent claims: 1. l-Phenylthio-3-alkylamino-2-propanols of the general formula I. CH ₂ -NH-R ₁ (I) 25th JO 35 in the Ri a straight or branched chain Ci- bis Cs-alkyl or cycloalkyl group, and their physiologically compatible acid addition salts. 2. Process for the preparation of the compounds of the formula I according to Claim 1, characterized in that in each case one is carried out in a manner known per se an amine of the formula H ₂ N - R, with an aryl glycide sulfide of the general formula II S-CH ₂ -CH- -CH ₂ (10 50 C-CH ₃ !!
ο or with a halohydrin in general Formula III CH ₂ -HaI 60 (III) C-CH, where Hal stands for chlorine. Bromine or iodine, implements, or b) a thiophenol of the general formula IV SH (IV) C-CH ₃ Il ο with a compound of the formula X-CH ₂ -NH - R, where X is for the / \ CH ₂ CH- or Y - CH ₃ - CH (OH) group (in which Y is a replaceable radical) stands, reacts, or c) a disulfide of the general formula V. S-S (V) under reducing conditions with the partners specified under b) to react brings, or d) an amino derivative of the formula VI S-CH ₂ -CH-CH ₂ -NH ₂ OH (Vl) C-CH ₃ Il ο can react with an alkyl halide of the formula Hal-Ri, where Rt has the same meaning has as in general formula I and the compounds I obtained, optionally in their physiologically compatible acid addition salts transferred. 3. Medicament, characterized by the content of a compound according to claim 1 in addition to common carriers and diluents. The invention relates to l- (2-acetylphenyl-. · Thio) -3-alkylamino-2-propanols of the general formula> |